A Therapeutic Uricase with Reduced Immunogenicity Risk and Improved Development Properties.
Humans and higher primates are unique in that they lack uricase, the enzyme capable of oxidizing uric acid. As a consequence of this enzyme deficiency, humans have high serum uric acid levels. In some people, uric acid levels rise above the solubility limit resulting in crystallization in joints, ac...
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doaj-c7112dc536a744a789e3b298aa48181d2020-11-24T20:45:59ZengPublic Library of Science (PLoS)PLoS ONE1932-62032016-01-011112e016793510.1371/journal.pone.0167935A Therapeutic Uricase with Reduced Immunogenicity Risk and Improved Development Properties.Andrew C NyborgChris WardAnna ZaccoBenoy ChackoLuba GrinbergJames C GeogheganRyan BeanMichaela WendelerFrank BartnikEllen O'ConnorFlaviu GruiaVidyashankara IyerHui FengVarnika RoyMark BergeJeffrey N MinerDavid M WilsonDongmei ZhouSimone NicholsonClynn WilkerChi Y WuSusan WilsonLutz JermutusHerren WuDavid A OwenJane OsbournSteven CoatsManuel BacaHumans and higher primates are unique in that they lack uricase, the enzyme capable of oxidizing uric acid. As a consequence of this enzyme deficiency, humans have high serum uric acid levels. In some people, uric acid levels rise above the solubility limit resulting in crystallization in joints, acute inflammation in response to those crystals causes severe pain; a condition known as gout. Treatment for severe gout includes injection of non-human uricase to reduce serum uric acid levels. Krystexxa® is a hyper-PEGylated pig-baboon chimeric uricase indicated for chronic refractory gout that induces an immunogenic response in 91% of treated patients, including infusion reactions (26%) and anaphylaxis (6.5%). These properties limit its use and effectiveness. An innovative approach has been used to develop a therapeutic uricase with improved properties such as: soluble expression, neutral pH solubility, high E. coli expression level, thermal stability, and excellent activity. More than 200 diverse uricase sequences were aligned to guide protein engineering and reduce putative sequence liabilities. A single uricase lead candidate was identified, which showed low potential for immunogenicity in >200 human donor samples selected to represent diverse HLA haplotypes. Cysteines were engineered into the lead sequence for site specific PEGylation and studies demonstrated >95% PEGylation efficiency. PEGylated uricase retains enzymatic activity in vitro at neutral pH, in human serum and in vivo (rats and canines) and has an extended half-life. In canines, an 85% reduction in serum uric acid levels was observed with a single subcutaneous injection. This PEGylated, non-immunogenic uricase has the potential to provide meaningful benefits to patients with gout.http://europepmc.org/articles/PMC5176304?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Andrew C Nyborg Chris Ward Anna Zacco Benoy Chacko Luba Grinberg James C Geoghegan Ryan Bean Michaela Wendeler Frank Bartnik Ellen O'Connor Flaviu Gruia Vidyashankara Iyer Hui Feng Varnika Roy Mark Berge Jeffrey N Miner David M Wilson Dongmei Zhou Simone Nicholson Clynn Wilker Chi Y Wu Susan Wilson Lutz Jermutus Herren Wu David A Owen Jane Osbourn Steven Coats Manuel Baca |
spellingShingle |
Andrew C Nyborg Chris Ward Anna Zacco Benoy Chacko Luba Grinberg James C Geoghegan Ryan Bean Michaela Wendeler Frank Bartnik Ellen O'Connor Flaviu Gruia Vidyashankara Iyer Hui Feng Varnika Roy Mark Berge Jeffrey N Miner David M Wilson Dongmei Zhou Simone Nicholson Clynn Wilker Chi Y Wu Susan Wilson Lutz Jermutus Herren Wu David A Owen Jane Osbourn Steven Coats Manuel Baca A Therapeutic Uricase with Reduced Immunogenicity Risk and Improved Development Properties. PLoS ONE |
author_facet |
Andrew C Nyborg Chris Ward Anna Zacco Benoy Chacko Luba Grinberg James C Geoghegan Ryan Bean Michaela Wendeler Frank Bartnik Ellen O'Connor Flaviu Gruia Vidyashankara Iyer Hui Feng Varnika Roy Mark Berge Jeffrey N Miner David M Wilson Dongmei Zhou Simone Nicholson Clynn Wilker Chi Y Wu Susan Wilson Lutz Jermutus Herren Wu David A Owen Jane Osbourn Steven Coats Manuel Baca |
author_sort |
Andrew C Nyborg |
title |
A Therapeutic Uricase with Reduced Immunogenicity Risk and Improved Development Properties. |
title_short |
A Therapeutic Uricase with Reduced Immunogenicity Risk and Improved Development Properties. |
title_full |
A Therapeutic Uricase with Reduced Immunogenicity Risk and Improved Development Properties. |
title_fullStr |
A Therapeutic Uricase with Reduced Immunogenicity Risk and Improved Development Properties. |
title_full_unstemmed |
A Therapeutic Uricase with Reduced Immunogenicity Risk and Improved Development Properties. |
title_sort |
therapeutic uricase with reduced immunogenicity risk and improved development properties. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2016-01-01 |
description |
Humans and higher primates are unique in that they lack uricase, the enzyme capable of oxidizing uric acid. As a consequence of this enzyme deficiency, humans have high serum uric acid levels. In some people, uric acid levels rise above the solubility limit resulting in crystallization in joints, acute inflammation in response to those crystals causes severe pain; a condition known as gout. Treatment for severe gout includes injection of non-human uricase to reduce serum uric acid levels. Krystexxa® is a hyper-PEGylated pig-baboon chimeric uricase indicated for chronic refractory gout that induces an immunogenic response in 91% of treated patients, including infusion reactions (26%) and anaphylaxis (6.5%). These properties limit its use and effectiveness. An innovative approach has been used to develop a therapeutic uricase with improved properties such as: soluble expression, neutral pH solubility, high E. coli expression level, thermal stability, and excellent activity. More than 200 diverse uricase sequences were aligned to guide protein engineering and reduce putative sequence liabilities. A single uricase lead candidate was identified, which showed low potential for immunogenicity in >200 human donor samples selected to represent diverse HLA haplotypes. Cysteines were engineered into the lead sequence for site specific PEGylation and studies demonstrated >95% PEGylation efficiency. PEGylated uricase retains enzymatic activity in vitro at neutral pH, in human serum and in vivo (rats and canines) and has an extended half-life. In canines, an 85% reduction in serum uric acid levels was observed with a single subcutaneous injection. This PEGylated, non-immunogenic uricase has the potential to provide meaningful benefits to patients with gout. |
url |
http://europepmc.org/articles/PMC5176304?pdf=render |
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